Phenytoin
Chemical
Hydantoin derivative
Use
- Tx seizures
- Anti-arrhythmias
- Trigeminal neuralgia tx
Presentation
Capsules
Colourless solution
50mg/mL
Dose / Route
PO 200 – 600mg/day
IV 15mg/kg (slow, over 1hr) LOAD
100mg TDS (maintenance)
Requires load because long t ½ → ∴ takes a while to reach steady state
Route
PO/IV
PO = slow absorption & unpredictable
Onset
IV immediate → peaks 1hr
PO unknown (variable) → Peaks 1 – 3hrs
MoA (mechanism)
- Binds & stabilises INACTIVE Na+ channels to prevent further generation of AP
- Potentiates GABA
- ↓Ca2+ influx → ∴ ↓excitability
Strong affinity for CNS binding
PD
CNS – stabilises membrane → prevents the spread of seizure
CVS
- Blocks fast Na+ channel
- ↓slope of Ph 0
- ↓amplitude of AP
- ∴ ↓ conduction velocity (-ve inotropy)
GI – ↓BGL, deranged LFTs
PK
*** Narrow therapeutic range: 10 = 20mcg/mL**
A
Slow but good
90% OBA
D
90% PPB high!
Always correct dose with [Albumin]
Low VD 0.6L/kg
M
Liver CYP450
Hydroxylation
- Saturable
- First order kinetics then ∆ Zero order kinetics
*** large genetic variation in rate of metabolism
Therapeutic dose & toxic dose are v. close ∴ requires monitoring
E
Metabolites in urine
t ½ B 9 – 24hrs
↓dose for hepatic impairment but not renal impairment
Adverse Effects
Idiosyncratic reactions
- Gum hyperplasia
- Hirsutism
- Megaloblastic AN
- Erythroderma
- SLE
Dose related reactions
- N&V
- Cerebral ataxia
- Nystagmus
- Dysarthria
- Tremor
Drug interactions
POTENT ENZYME INDUCER
- ↓effectiveness BZD, pethidine, warfarin
- ↑LA CNS toxicity
- ↑dose of NMBD (except atrac req)
- Isoniazid & metronidazole (enzyme inhibitors) will ↑risk phenytoin toxicity
Teratogenic